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输血相关微嵌合体

Transfusion-associated microchimerism.

作者信息

Utter G H, Reed W F, Lee T-H, Busch M P

机构信息

Department of Surgery, UC, Davis Medical Center, Sacramento, CA 95817, USA.

出版信息

Vox Sang. 2007 Oct;93(3):188-95. doi: 10.1111/j.1423-0410.2007.00954.x.

Abstract

Blood transfusion is a newly recognized cause of microchimerism, the stable persistence of a minor population of allogeneic cells. Relatively recent advances in polymerase chain reaction technology have spawned new information about the frequency and aetiology of transfusion-associated microchimerism (TA-MC). Although conceptually related to fetal-maternal microchimerism, TA-MC is a distinct and separate entity. Evidence of TA-MC has been strongest among patients with severe traumatic injuries who receive relatively fresh blood products shortly after an episode of massive haemorrhage. The presence of a focal deficit in the cellular immunologic repertoire prior to transfusion that happens to match a blood donor's human leucocyte antigen type also appears to be an important predisposing factor. TA-MC seems to be common (affecting approximately 10% of transfused injured patients), enduring (lasting years to decades) and pronounced (involving up to 5% of circulating leucocytes and multiple immunophenotypic lineages suggestive of haematopoietic engraftment). Further study of this topic may reveal important information regarding potential clinical consequences of TA-MC, as well as basic haematologic and immunologic processes.

摘要

输血是微嵌合体(即少量异基因细胞的稳定持续存在)一种新发现的成因。聚合酶链反应技术最近取得的进展催生了有关输血相关微嵌合体(TA-MC)的频率及病因的新信息。尽管TA-MC在概念上与胎儿-母体微嵌合体相关,但它是一个独特且独立的实体。在严重创伤性损伤患者中,TA-MC的证据最为确凿,这些患者在大量出血事件后不久接受了相对新鲜的血液制品。输血前细胞免疫库中恰好与献血者人类白细胞抗原类型相匹配的局灶性缺陷的存在似乎也是一个重要的易感因素。TA-MC似乎很常见(约10%的输血受伤患者受其影响)、持久存在(持续数年至数十年)且程度显著(涉及高达5%的循环白细胞以及多个提示造血植入的免疫表型谱系)。对该主题的进一步研究可能会揭示有关TA-MC潜在临床后果以及基础血液学和免疫学过程的重要信息。

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